疑似肾细胞癌的肾肿块患者术前可检测到的肿瘤信息循环肿瘤 DNA 的相关肿瘤特征

IF 5.3 2区 医学 Q1 ONCOLOGY
JCO precision oncology Pub Date : 2024-09-01 Epub Date: 2024-09-30 DOI:10.1200/PO.24.00281
Reuben Ben-David, Parissa Alerasool, Hitasha Kalola, Neeraja Tillu, Mohammed Almoflihi, Che-Kai Tsao, Matthew D Galsky, John P Sfakianos, Peter Wiklund, Nikhil Waingankar, Reza Mehrazin
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引用次数: 0

摘要

目的:了解与肾细胞癌(RCC)患者体内可检测到的循环肿瘤 DNA(ctDNA)相关的特定肿瘤特征对于今后旨在确定此类检测的临床实用性的研究至关重要。我们对怀疑为RCC的肾肿块患者术前检测到的ctDNA的相关病理和临床特征进行了描述:2022-2023年期间,因非转移性疑似RCC(cT1b-T3)而接受肾部分或根治性切除术的连续患者在术前和术后进行了前瞻性肿瘤信息ctDNA分析。研究采用描述性统计和单变量分析来描述研究结果:69名患者的中位年龄为62岁(IQR,51-70),中位随访时间为7个月(IQR,3-11),共收集了205份ctDNA样本进行分析。在 64 名患者中,39 人(61%)术前可检测到 ctDNA。有 47 名患者的术后 ctDNA 状态可用,其中 3 人(6%)可检测到 ctDNA。其中两人受累于下腔静脉(IVC),一人出现转移性疾病。对单纯恶性RCC(n = 65)进行的亚组分析显示,术前检测到ctDNA的患者病理分期更高(P = .001),肿瘤更大(7 v 4.5 cm; P = .001),肿瘤复杂程度更高(P = .022),肿瘤3-4级的比例更高(P = .038)。病理结果显示,所有肾静脉或 IVC 严重受累(9 例)和淋巴管受侵(6 例)的患者术前都能检测到 ctDNA。单变量分析发现,肿瘤复杂程度高、肿瘤较大和肿瘤分级3-4级是术前检测到ctDNA的预测因素:结论:61%的非转移性RCC患者术前可检测到ctDNA,且ctDNA与临床相关特征相关。临床试验应考虑结合术前和术后的ctDNA分析,以增强对疾病复发的预测并完善治疗决策。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Tumor Characteristics Associated With Preoperatively Detectable Tumor-Informed Circulating Tumor DNA in Patients With Renal Masses Suspicious for Renal Cell Carcinoma.

Purpose: Understanding the specific tumor characteristics associated with detectable circulating tumor DNA (ctDNA) in patients with renal cell carcinoma (RCC) is critical for informing future studies aiming to establish the clinical utility of such testing. We characterized the pathologic and clinical features associated with preoperatively detectable ctDNA in patients with renal masses suspicious for RCC.

Methods: Consecutive patients who underwent partial or radical nephrectomy for nonmetastatic suspected RCC (cT1b-T3) during 2022-2023 had prospectively collected tumor-informed ctDNA analyses conducted preoperatively and postoperatively. Descriptive statistics and univariate analyses were used to describe the study findings.

Results: Sixty-nine patients with a median age of 62 years (IQR, 51-70) and a median follow-up time of 7 months (IQR, 3-11) had 205 ctDNA samples collected for analysis. Thirty-nine (61%) had preoperative detectable ctDNA of 64 patients. Postoperative ctDNA status was available for 47 patients, and three (6%) had detectable ctDNA. Two had inferior vena cava (IVC) involvement, and one developed metastatic disease. Subgroup analysis of solely malignant RCC (n = 65) revealed that patients with preoperative detectable ctDNA had a higher pathologic stage (P = .001), larger tumors (7 v 4.5 cm; P = .001), higher tumor complexity (P = .022), and increased rates of tumor grades 3-4 (P = .038). All patients with gross renal vein or IVC involvement (n = 9) and those with lymphovascular invasion (n = 6) on pathology had detectable preoperative ctDNA. On univariate analysis, high tumor complexity, larger tumors, and tumor grades 3-4 were found to be predictors of preoperatively detectable ctDNA status.

Conclusion: Preoperative ctDNA was detectable in 61% of patients with nonmetastatic RCC, and it correlated with clinically relevant features. Clinical trials should consider incorporating both preoperative and postoperative ctDNA analyses to augment prediction of disease recurrence and to refine treatment decision making.

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